Tg(INS-SOD2)3Pne Transgene Detail MGI Mouse (MGI:3525180)

Tg(INS-SOD2)3Pne
Transgene Detail

Summary

Symbol:	Tg(INS-SOD2)3Pne
Name:	transgene insertion 3, Paul N Epstein
MGI ID:	MGI:3525180
Synonyms:	IsNOD, MnSOD3
Transgene:	Tg(INS-SOD2)3Pne Location: unknown
Alliance:	Tg(INS-SOD2)3Pne page

Transgene
origin

Strain of Origin:

FVB

Transgene
description

Transgene Type:

Transgenic (Humanized sequence, Inserted expressed sequence)

Mutation:

Insertion

Tg(INS-SOD2)3Pne expresses 1 gene

Mutation details: The transgene expresses the full-length human mitochondrial superoxide dismutase cDNA controlled by the human insulin promoter. Immunohistochemical staining with mitochondrial superoxide dismutase specific antibody confirms transgene expression localized to the mitochondria of pancreatic islet cell. (J:97839)

Phenotypes

View phenotypes and curated references for all genotypes (concatenated display).

Disease models

Find Mice (IMSR)

Mouse strains and cell lines available from the International Mouse Strain Resource (IMSR)
Carrying this Mutation:	Mouse Strains: 1 strain available Cell Lines: 0 lines available

Notes

Five transgenic lines were generated on an FVB background. This line expressed the highest SOD2 activity.

Transgenic mice are viable, fertile, normal in size, and do not display any gross physical or behavioral abnormalities. There is an approximately 10 fold increase in SOD2 activity in transgenic islets when compared to wild-type controls. There is no statistical difference in insulin and DNA content, insulin staining and islet morphology or diabetes development following cyclophosphamide treatment between mutant and wild-type NOD mice. Transgenic mice are resistant to diabetes when treated with streptozotocin. Islet beta cells from transgenics generate less ROS when treated with peroxynitrite or superoxide. Untreated mutants do not display accelerated spontaneous diabetes.

References

Original:	J:97839 Chen H, et al., MnSOD and catalase transgenes demonstrate that protection of islets from oxidative stress does not alter cytokine toxicity. Diabetes. 2005 May;54(5):1437-46
All:	3 reference(s)

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